| Literature DB >> 34428278 |
Nathanael R Fillmore1,2, Diana Cirstea3,2, Anusha Munjuluri1,3, Hassan Yameen4, Sarvari V Yellapragada5,6, Nhan V Do1,7, Mary T Brophy1,7, Raphael E Szalat1,7, Nikhil C Munshi1,2.
Abstract
Multiple myeloma (MM) is a heterogeneous disease that has an increased incidence in African Americans (AAs). We previously observed that, with equal access to health care, younger AA patients (age < 65 years) have superior overall survival (OS) compared with younger White patients. Because MM prognosis is influenced by 17p deletion (del17p), we investigated racial differences in its occurrence and impact in a large cohort of MM patients from the Veterans Affairs (VA) system. Among 2243 VA patients with MM for whom del17p data were available, del17p was present in 8.83% of all patients, with a significantly lower prevalence in AAs (5.56%) compared with Whites (10.52%; P < .001). The difference was even more pronounced among younger AAs (<65 years) vs younger Whites (4.34% vs 9.8%, respectively; P = .004). However, we did not observe any significant difference in survival between AA and White patients with del17p, regardless of age category, suggesting that del17p carries a poor prognosis across race and age. Interestingly, among patients without del17p, we still noted a significantly superior OS in younger AAs compared with younger Whites (7.75 vs 5.10 years; P = .042). Our study shows a lower incidence of del17p in AAs but suggests that the survival advantage for younger AAs is primarily due to factors other than del17p.Entities:
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Year: 2021 PMID: 34428278 PMCID: PMC8945588 DOI: 10.1182/bloodadvances.2020004001
Source DB: PubMed Journal: Blood Adv ISSN: 2473-9529